Abnormal expression of CCNDI and RBI in resection margin epithelia of lung cancer patients

Betticher, Daniel; Heighway, Jim; Thatcher, Nick; Hasleton, Philip

doi:10.1038/bjc.1997.300

Cited by 45 publications

(30 citation statements)

References 36 publications

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“…As other authors observed, the intensity of Ki67 expression is also higher in dysplasia. This way, we reinforce the utility of Ki67 as a biomarker, namely for dysplasia, as it appears as a group characterized by high proliferative index, subscribing the literature and other authors' study of preneoplastic lesions [22][23][24][25][26]59]. P53, the "guardian" maintaining the integrity of the genome by participating in the DNA damage checkpoints in the cell cycle, regulating cellular proliferation and apoptosis [20], has been detected in preneoplastic lesions of the lung, suggesting that it occurs early during lung carcinogenesis [14,18,20] as the obtained results confirmed.…”

Section: Discussionmentioning

confidence: 84%

“…[18][19][20]. Those genomic and molecular abnormalities are early events in lung carcinogenesis and can persist in bronchial lesions for months or years and their persistence or regression have been correlated with lesions' evolution [15,[21][22][23][24][25][26][27][28][29][30]. Molecular changes are recognized not only in lung cancer, but also in bronchial epithelium and parenchyma of current and former smokers without the development of lung cancer [31,32].…”

Section: Introductionmentioning

confidence: 99%

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EGFR/erB-1, HER2/erB-2, CK7, LP34, Ki67 and P53 expression in preneoplastic lesions of bronchial epithelium: an immunohistochemical and genetic study

et al. 2011

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A prognostic interpretation of preneoplastic lesions would have impact in bronchial carcinoma early diagnosis and through the study of Erb-B family receptors as they have an important role in lung carcinogenesis. The existence of drugs as tyrosine kinase inhibitors stressed the importance of studying gene alterations for selected chemoprevention schemes and characterization of carcinogenesis. Bronchial preneoplastic lesions were characterized by immunohistochemistry using the antibodies LP34 (high weigh molecular cytokeratin), CK7, chromogranin A, Ki67, p53, C-erbB-2 and EGFR. HER2 and EGFR gene copy number was also evaluated by fluorescent in situ hybridization in those lesions. The expected results defined the origin cell for basal cell hyperplasia and squamous metaplasia as adaptative lesions and dysplasia. By known experiences and published data, beyond the stem cell, the spectral evolution of bronchial preneoplastic lesions was demonstrated by characterizing basal cells (LP34) and their neoplastic potentiality. Dysplasias showed a higher expression of EGFR, Ki67 and p53 with a stepwise increase with the gravity of the respective grading. C-erbB-2 immunohistochemical overexpression was a rare event in preneoplastic lesions. Polysomy was the main mechanism for EGFR and HER2/ neu higher gene copy number and together with increased proliferation index (Ki67) will account to preview bronchial carcinogenesis.

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Section: Discussionmentioning

confidence: 84%

Section: Introductionmentioning

confidence: 99%

EGFR/erB-1, HER2/erB-2, CK7, LP34, Ki67 and P53 expression in preneoplastic lesions of bronchial epithelium: an immunohistochemical and genetic study

et al. 2011

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“…The basal cells are multipotent reserve cells that retain the capacity to generate the various differentiated cell types of the airway epithelium. NSCLCs arise from a component(s) of this airway epithelium and it is generally possible to identify a range of pre-neoplastic lesions in the bronchial epithelia of patients, particularly smokers (Betticher et al, 1997;Ratschiller et al, 2003). Examination of multiple tumour-free sites from 20 patients allowed us to make two potentially significant observations related to the pathological expression of maspin.…”

Section: Discussionmentioning

confidence: 99%

Maspin – the most commonly-expressed gene of the 18q21.3 serpin cluster in lung cancer – is strongly expressed in preneoplastic bronchial lesions

et al. 2003

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Maspin, SCCA1/2 and hurpin were identified by cDNA microarray analyses as dramatically differentially expressed transcripts in primary non-small cell lung cancer (NSCLC). These sequences are located within a 10-gene serpin cluster on 18q21.3. Using comparative RT-PCR, we have investigated the expression of each of these serpins, including their flanking loci, in an independent NSCLC series. Whereas six of the genes (maspin, SCCA1, SCCA2, hurpin, megsin and pAI-2) were commonly differentially expressed in primary lesions, each significantly more often in squamous cell tumours, maspin was identified as the most frequently overrepresented sequence in both squamous cell carcinoma and adenocarcinoma. Using a well-characterized monoclonal antibody, we have shown strong maspin expression in tumour protein extracts, detected multiple isoforms of the 42 kDa protein and shown that maspin is localized specifically to the tumour cells within neoplastic lesions. In contrast, most cells in non-neoplastic lung tissue appear not to express the gene, with the exception of the multipotent basal epithelial cells that line the bronchial airway. These reserve cells generally show strong predominantly nuclear localization of maspin. Strong nuclear expression of maspin within primary tumour cells is correlated with increased survival (P ¼ 0.05) and a longer remission duration (P ¼ 0.02) in resectable-staged patients. However, within the airways of cancer patients and somewhat in contrast to this observation, such expression was more frequently detected in the superficial cells of preneoplastic over non-neoplastic epithelia (Po0.0001), consistent with a role for the protein in early neoplasia.

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“…(6,7). Overexpression of cyclin D1 is a frequent and early step in lung carcinogenesis (8)(9)(10)(11). Cyclin D1 overexpression is often associated with gene amplification (12) as well as allele-specific expression imbalance (11).…”

Section: Introductionmentioning

confidence: 99%

Retinoid Targeting of Different D-Type Cyclins through Distinct Chemopreventive Mechanisms

Ma¹,

Feng²,

Sekula³

et al. 2005

Cancer Research

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D-type cyclins (cyclins D1, D2, and D3) promote G 1 -S progression and are aberrantly expressed in cancer. We reported previously that all-trans-retinoic acid chemoprevented carcinogenic transformation of human bronchial epithelial (HBE) cells through proteasomal degradation of cyclin D1. Retinoic acid is shown here to activate distinct mechanisms to regulate different D-type cyclins in HBE cells. Retinoic acid increased cyclin D2, decreased cyclin D3 and had no effect on cyclin D1 mRNA expression. Retinoic acid decreased cyclin D1 and cyclin D3 protein expression. Repression of cyclin D3 protein preceded that of cyclin D3 mRNA. Proteasomal inhibition prevented the early cyclin D3 degradation by retinoic acid. Threonine 286 (T286) mutation of cyclin D1 stabilized cyclin D1, but a homologous mutation of cyclin D3 affecting threonine 283 did not affect cyclin D3 stability, despite retinoic acid treatment. Lithium chloride and SB216763, both glycogen synthase kinase 3 (GSK3) inhibitors, inhibited retinoic acid repression of cyclin D1, but not cyclin D3 proteins. Notably, phospho-T286 cyclin D1 expression was inhibited by lithium chloride, implicating GSK3 in these effects. Expression of cyclin D1 and cyclin D3 was deregulated in retinoic acid-resistant HBE cells, directly implicating these species in retinoic acid response. D-type cyclins were independently targeted using small interfering RNAs. Repression of each D-type cyclin suppressed HBE growth. Repression of all D-type cyclins cooperatively suppressed HBE growth. Thus, retinoic acid repressed cyclin D1 and cyclin D3 through distinct mechanisms. GSK3 plays a key role in retinoid regulation of cyclin D1. Taken together, these findings highlight these cyclins as molecular pharmacologic targets for cancer chemoprevention. (Cancer Res 2005; 65(14): 6476-83)

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Abnormal expression of CCNDI and RBI in resection margin epithelia of lung cancer patients

Cited by 45 publications

References 36 publications

EGFR/erB-1, HER2/erB-2, CK7, LP34, Ki67 and P53 expression in preneoplastic lesions of bronchial epithelium: an immunohistochemical and genetic study

EGFR/erB-1, HER2/erB-2, CK7, LP34, Ki67 and P53 expression in preneoplastic lesions of bronchial epithelium: an immunohistochemical and genetic study

Maspin – the most commonly-expressed gene of the 18q21.3 serpin cluster in lung cancer – is strongly expressed in preneoplastic bronchial lesions

Retinoid Targeting of Different D-Type Cyclins through Distinct Chemopreventive Mechanisms

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